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复发多发性骨髓瘤中针对 BCMA 的嵌合抗原受体 T 细胞反应和耐药的单细胞多组学剖析。

Single-cell multiomic dissection of response and resistance to chimeric antigen receptor T cells against BCMA in relapsed multiple myeloma.

机构信息

Fraunhofer Institute for Cell Therapy and Immunology IZI, Leipzig, Germany.

Department of Hematology, Cellular Therapy and Hemostaseology, University Hospital of Leipzig, Leipzig, Germany.

出版信息

Nat Cancer. 2024 Sep;5(9):1318-1333. doi: 10.1038/s43018-024-00763-8. Epub 2024 Apr 19.

Abstract

Markers that predict response and resistance to chimeric antigen receptor (CAR) T cells in relapsed/refractory multiple myeloma are currently missing. We subjected mononuclear cells isolated from peripheral blood and bone marrow before and after the application of approved B cell maturation antigen-directed CAR T cells to single-cell multiomic analyses to identify markers associated with resistance and early relapse. Differences between responders and nonresponders were identified at the time of leukapheresis. Nonresponders showed an immunosuppressive microenvironment characterized by increased numbers of monocytes expressing the immune checkpoint molecule CD39 and suppressed CD8 T cell and natural killer cell function. Analysis of CAR T cells showed cytotoxic and exhausted phenotypes in hyperexpanded clones compared to low/intermediate expanded clones. We identified potential immunotherapy targets on CAR T cells, like PD1, to improve their functionality and durability. Our work provides evidence that an immunosuppressive microenvironment causes resistance to CAR T cell therapies in multiple myeloma.

摘要

预测复发/难治性多发性骨髓瘤嵌合抗原受体 (CAR) T 细胞反应和耐药的标志物目前尚缺乏。我们对接受已批准的 B 细胞成熟抗原导向 CAR T 细胞治疗前后分离的外周血和骨髓单核细胞进行单细胞多组学分析,以鉴定与耐药和早期复发相关的标志物。在白细胞分离时鉴定出反应者和无反应者之间的差异。无反应者表现出免疫抑制微环境的特征,表现为表达免疫检查点分子 CD39 的单核细胞数量增加,并且抑制 CD8 T 细胞和自然杀伤细胞功能。CAR T 细胞分析显示,与低/中扩增克隆相比,超扩增克隆具有细胞毒性和耗竭表型。我们鉴定了 CAR T 细胞上的潜在免疫治疗靶点,如 PD1,以改善其功能和持久性。我们的工作提供了证据,表明免疫抑制微环境导致多发性骨髓瘤对 CAR T 细胞治疗产生耐药性。

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